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Genetic Hearing Loss

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Genetic Hearing Loss

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    1. 1 Genetic Hearing Loss Jing Shen M.D. Ronald Deskin M.D. UTMB Dept of Otolaryngology March 2004

    2. 2 Epidemiology Hearing loss occurs in 1 out of every 1,000 births 50 % are hereditary Syndromic vs. nonsyndromic 30% syndromic 70% nonsyndromic Autosomal dominant vs. autosomal recessive vs. x-linked vs. mitochondrion

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    6. 6 Methods Linkage mapping Mouse model Difficulties: Families too small for linkage analysis Assortive mating introducing various genes into one single pedigree Incomplete penetrance

    7. 7 Syndromic deafness Has other abnormalities About 20-30% of genetic hearing loss Two syndromes can be caused by different mutations of the same gene Mutations of more than one gene can cause the same clinical phenotype

    8. 8 Alport syndrome At least 1% of congenital hearing loss X-linked inheritance (80%), autosomal recessive as well as dominant Sensorineural hearing loss: mostly affect high tone Renal dysfunction Microscopic hematuria Man are more severely affected than woman Onset in early childhood and progress to renal failure in adulthood increased risk of developing anti-GBM nephritis after renal transplantation

    9. 9 Alport syndrome Ocular abnormalities Lenticulus Retina flecks Defective collagen type 4 causes abnormalities in the basement membrane 3 genes: COL4A5, COL4A3, COL4A4 These collagens found in the basilar membrane, parts of the spiral ligament, and stria vascularis Exact mechanism of hearing loss is unknown loss of integrity of the basement membrane might affect adhesion of the tectorial membrane, and in the basilar membrane and its junction with the spiral ligament, translation of mechanical energy may be affected loss of integrity of the basement membrane might affect adhesion of the tectorial membrane, and in the basilar membrane and its junction with the spiral ligament, translation of mechanical energy may be affected

    10. 10 Branchio-oto-renal syndrome 2% of profoundly deaf children Autosomal dominant disorder Otologic anomalies: variable hearing loss (sensorineural, conductive or mixed) malformed pinna, preauricular pits Branchial derived abnormalities: cyst, cleft, fistula Renal malformation: renal dysplasia with anomalies of the collecting system, renal agenesis Sometimes with lacrimal duct abnormalities: aplasia, stenosis EYA1 gene mutation – knockout-mice showed no ears and kidneys because apoptotic regression of the organ primordia 90% has hearing loss, 80% with ear pit, 60% with brachial cyst, 15% with renal anomalies. 90% has hearing loss, 80% with ear pit, 60% with brachial cyst, 15% with renal anomalies.

    11. 11 Jervell and Lange-Nielsen syndrome Autosomal recessive 0.25% of profound congenital hearing loss Prolonged QT interval, sudden syncopal attacks Severe to profound sensorineural hearing loss 2 genes identified: KVLQT1: expressed in the stria vascularis of mouse inner ear KCNE1 Both gene products form subunits of a potassium channel involved in endolymph homeostasis KVLQT heterozygous has no hearing loss, only has prolonged QT interval KVLQT heterozygous has no hearing loss, only has prolonged QT interval

    12. 12 Norrie syndrome X-linked inheritance Ocular symptoms with congenital blindness: pseudotumor of the retina, retinal hyperplasia, hypoplasia and necrosis of the inner layer of the retina, cataracts, phthisis bulbi Progressive sensorineural hearing loss Mental deficiency Norrin gene: encodes a protein related to mucins Phthisis bulbi: atrophy and degeneration of a blind eyePhthisis bulbi: atrophy and degeneration of a blind eye

    13. 13 Pendred Syndrome Most common form of syndromal deafness- 4-10 % Autosomal recessive disorder Sensorineural hearing loss bilateral, severe to profound, and sloping in the higher frequencies incomplete partition of the cochlear

    14. 14 Pendred syndrome Vestibular dysfunction: enlargement of the vestibular aqueducts, the endolymphatic sac and duct Thyroid goiter: usually euthyroid, can be hypothyroid defective organic binding of iodine positive potassium perchlorate discharge test

    15. 15 Pendred syndrome PDS gene mutations: on chromosome 7q31 encodes pendrin: an anion transporter in inner ear, thyroid, kidney PDS knockout mouse: complete deaf endolymph-containing spaces enlargement inner and outer hair cell degeneration no thyroid abnormality

    16. 16 Stickler syndrome Autosomal dominant Variable sensorineural hearing loss Ocular symptoms: progressive myopia, resulting in retina detachment and blindness Arthropathy: premature degenerative changes in various joints Orofacial features: midface hypoplasia Three genes: COL2A1, COL11A1, COL11A2 Associated with defective collagen protein Each gene mutation corresponding to a phenotype Originally described by stickler: ocular symptoms, arthropathy. Type 3 has no ocular symptoms. Originally described by stickler: ocular symptoms, arthropathy. Type 3 has no ocular symptoms.

    17. 17 Treacher-collins syndrome Autosomal dominant with variable expression Conductive hearing loss Craniofacial abnormalities: Coloboma of the lower lids, micrognathia, microtia, hypoplasia of zygomatic arches, macrostomia, slanting of the lateral canthi TCOF1 gene: Involved in nucleolar-cytoplasmic transport mutation results in premature termination of the protein product

    18. 18 Usher syndrome Autosomal recessive disorder Sensorineural hearing loss Progressive loss of sight due to retinitis pigmentosa Three different clinical types 11 loci and 6 genes have been identified

    19. 19 Usher syndrome Type 1: Profound congenital deafness, absent vestibular response, onset of retinitis pigmentosa in the first decade of life Type 2: Sloping congenital deafness, normal vestibular response, onset of retinitis pigmentosa in first or second decade of life Type 3: Progressive hearing loss, variable vestibular response, variable onset of retinitis pigmentosa

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    21. 21 Usher syndrome MYO7A: encodes for myosin 7A, molecular motor for hair cells USH1C: encodes for harmonin, bundling protein in stereocilia CDH23: encodes cadherin 23, an adhesion molecule may be important for crosslinking of stereocilia, also may be involved in maintaining the ionic composition of the endolymph Myosin 7A, harmonin, and cadherin 23 form a transient functional complex in stereocilia In mouse model, preserving the shapes of the individual stereocilia as well as shaping the stereocilia bundle during mouse development.In mouse model, preserving the shapes of the individual stereocilia as well as shaping the stereocilia bundle during mouse development.

    22. 22 Waardenburg syndrome About 2% of congenital hearing loss Usually autosomal dominant Dystonia canthorum Pigmentary abnormalities of hair, iris and skin Sensorineural hearing loss 4 clinical subtypes

    23. 23 Waardenburg syndrome Type 1: With dystopia canthorum Penetrance for hearing loss 36% to 58% Wide confluent eyebrow, high broad nasal root, heterochromia irides, brilliant blue eyes, premature gray of hair, eyelashes, or eyebrows, white forelock, vestibular dysfunction Type 2: like type 1 but without dystopia canthorum Hearing loss penetrance as high as 87%

    24. 24 Waardenburg syndrome Type 3 (Klein-Waardenburg syndrome): Type 1 clinical features + hypoplastic muscles and contractures of the upper limbs Type 4 ( Shah-Waardenburg syndrome): Type 2 clinical features + Hirschsprung’s disease Five genes on five chromosomes have been identified

    25. 25 Waardenburg syndrome Type 1 and type 3: all associated with PAX3 gene mutation Type 2: Associated with dominant mutations of MITF gene Associated with homozygous deletion of SLUG gene MITF was found to activate the SLUG gene Pax3 for determining neural crest cell fate in the developing nervous system. Type 2 is heterogeneous. Mitf (microphthalmia gene)– transcription factor. slug transcription factor for differentiation of melanocytes. Mutation of mitf fail to properly activate slug. Mouse model of slug showed areas of depigmentation. Pax3 for determining neural crest cell fate in the developing nervous system. Type 2 is heterogeneous. Mitf (microphthalmia gene)– transcription factor. slug transcription factor for differentiation of melanocytes. Mutation of mitf fail to properly activate slug. Mouse model of slug showed areas of depigmentation.

    26. 26 Waardenburg syndrome Type 4: EDNRB gene – encodes endothelin-b receptor, development of two neural crest derived-cell lineages, epidermal melanocytes and enteric neurons EDN3 gene – encodes endothelin-3, ligand for the endothelin-b receptor SOX10 gene – encodes transcription factor

    27. 27 Non-syndromic deafness About 70-80% of hereditary hearing loss Autosomal dominant (15%): 41 loci (DFNA) and 20 genes identified Usually postlingual onset, progressive Severity from moderate to severe Majority of the hearing loss in middle, high or all frequencies Autosomal recessive (80%): 33 loci (DFNB) and 21 genes identified Usually prelingual onset, non-progressive Severity from severe to profound All frequencies affected X-linked (2-3%): 4 loci (DFN) and 1 gene identified Either high or all frequencies affected See hereditary hearing loss homepage for all listed loci and genes.See hereditary hearing loss homepage for all listed loci and genes.

    28. 28 Non-syndromic deafness Identified genes encode: Unconventional myosin and cytoskeleton proteins Extracellular matrix proteins Channel and gap junction components Transcription factors Proteins with unknown functions More than one gene found in the same loci (DFNA2 and DFNA3) Some genes cause autosomal dominant and autosomal recessive hearing loss Some genes cause non-syndromic and syndromic hearing loss For ex: GJB2: dominant mutation cause wild-type unable to form channels. Recessive mutation cause decreased channel activity.For ex: GJB2: dominant mutation cause wild-type unable to form channels. Recessive mutation cause decreased channel activity.

    29. 29 Ion homeostasis Potassium recycling to maintain high potassium concentration in endolymph KCNQ4: encodes a potassium channel SLC26A4: encodes an anion transporter, pendrin 4 gap junction genes: GJB2, GJB3, DJB6, GJA1 Encode connexin proteins Function of gap junctions: molecular pores connecting two adjacent cells allowing small molecules and metabolites exchange

    30. 30 GJB2 (Gap Junction Beta 2) The first non-syndromic sensorineural deafness gene to be discovered On chromosome 13q11 50% of recessive non-syndromic hearing loss Encodes connexin 26 Expressed in stria vascularis, basement membrane, limbus, spiral prominence of cochlea Recycling of potassium back to the endolymph after stimulation of the sensory hair cell 80 recessive and 6 dominant mutations 35delG mutation One guanosine residue deletion from nucleotide position 35 Results in protein truncation High prevalence in Caucasian population Screening test available

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    33. 33 Transcription factors POU3F4 X-linked mixed hearing loss Stapes fixation causing conductive hearing loss Increased perilymphatic pressure Causing the typical “gusher” during stapes footplate surgery – stapes-gusher syndrome POU4F3 Autosomal dominant hearing loss Knockout mice fail to develop hair cells with subsequent loss of spiral and vestibular ganglia EYA4 TFCP2L3

    34. 34 Cytoskeleton proteins Associated with actin-rich stereocilia of hair cells Myosin: actin-dependent molecular motor proteins MYH9 MYO3A, MYO6, MYO7A, MYO15 – all have vestibular dysfunction Otoferlin: calcium triggered synaptic vesicle trafficking OTOF one particular mutation accounts for 4.4% of recessive prelingual hearing loss negative for GJB2 mutation Actin-polymerization protein: HDIA1 Harmonin: organize multiprotein complexes in specific domains (tight junction, synaptic junction) USH1C (also in Usher type 1c) Cadherin: important for stereocilia organization CDH23 ( also in Usher type 1d)

    35. 35 Extracellular matrix components TECTA Encodes alpha tectorin- component of the tectorial membrane Knockout mice with detachment of tectorial membrane from the cochlear epithelium COL11A2 Encodes collage type XI polypeptide subunit 2 Knockout mice with atypical and disorganized collagen fibrils of the tectorial membrane COCH Encodes COCH (coagulation factor C homologue) protein Expressed in cochlear and vestibular organs Associated with vestibular problems Tectorial membrane overlying the hair cell , bend the stereocilia and open the channels. 25% pt with coch mutation noted to have some meniere’s symptoms: tinnitus, vertigo, pressure feeling in the ear. Tectorial membrane overlying the hair cell , bend the stereocilia and open the channels. 25% pt with coch mutation noted to have some meniere’s symptoms: tinnitus, vertigo, pressure feeling in the ear.

    36. 36 Unknown function genes WFS1 Dominant sensorineural hearing loss Responsible for 75% of low frequency nonsyndromic progressive hearing Responsible for up to 90% of cases of Wolfram syndrome, a recessive disorder with diabetes mellitus, diabetes insipidus, optic atrophy, and deafness

    37. 37 Mitochondrial disorders 2-10 mitochondrial chromosomes in each mitochondrion Transmitted only through mothers With syndromic hearing loss Associated with systemic neuromuscular syndromes: such as Kearns-Sayre syndrome, MELAS, MERRF Also in families with diabetes and sensorineural hearing loss Associated with skin condition: palmoplantar keratoderma With non-syndromic hearing loss With aminoglycoside ototoxic hearing loss A1555G mutation in the 12S ribosomal RNA gene Maternally transmitted predisposition to aminoglycoside ototoxicity Accounts for 15% of all aminoglycoside induced deafness MELAS: mitochondrial encephalomyopathy, lactic acidosis, stroke-like episodes MERRF: mitochondrial encephalomyopathy with ragged red fibersMELAS: mitochondrial encephalomyopathy, lactic acidosis, stroke-like episodes MERRF: mitochondrial encephalomyopathy with ragged red fibers

    38. 38 Evaluation History Prenatal: infection, medication Perinatal: risk factors Postnatal: infection, speech and language milestones Family: hearing loss in first and second degree relatives Hearing loss occurred before age 30 Consanguinity or common origin from ethnically isolated areas Risk factors: low birth weight, prematurity, time in NICU, hyperbilirubinemia, sepsis, ototoxic medications, birth hypoxiaRisk factors: low birth weight, prematurity, time in NICU, hyperbilirubinemia, sepsis, ototoxic medications, birth hypoxia

    39. 39 Evaluation Physical exam: features of syndromic hearing loss Hair color: white forelock, premature graying Facial shape Skull shape Eye: color, position, intercanthal distance, cataracts, retinal findings Ear: preauricular pit, skin tags, shape and size of pinna, abnormality of EAC and TM Oral cavity: cleft Neck: brachial anomalies, thyroid enlargement Skin: hyper/ hypopigmentation, café-au-lait spots Digits: number, size, shape Neurological exam: gait, balance Ophthalmology exam: ERG (electroretinography) uncover early retinitis pigmentosaOphthalmology exam: ERG (electroretinography) uncover early retinitis pigmentosa

    40. 40 Evaluation Audiologic evaluation Lab testing: based on history and physical exam Torch titers CBC and electrolytes Urinalysis thyroid function test (perchlorate discharge test) EKG Radiological study: CT temporal bone is the test of choice Dilated vestibular aqueduct (>1.5mm at middle third or >2mm anywhere along its length) Mondini malformation Semicircular canal absence or dysplasia Internal auditory canal narrowing or dilation Renal ultrasound Cbc: fechtner syndrome/epstein syndrome Electorlyte: renal dysfunction Dilated vestibular aqueduct : suggest pendred and BOR. Need to eval for pendred syndrome Semicircle.: Charge syndrome Stape-gusher syndrome Cbc: fechtner syndrome/epstein syndrome Electorlyte: renal dysfunction Dilated vestibular aqueduct : suggest pendred and BOR. Need to eval for pendred syndrome Semicircle.: Charge syndrome Stape-gusher syndrome

    41. 41 Genetic screening GJB2 most common cause of severe to profound nonsyndromic recessive deafness High prevalence of 35delG mutation Small size of GJB2 gene SLC26A4- most common cause of Mondini dysplasia or dilated vestibular aqueduct syndrome EYA1- 30-40% of families with a branchio-oto-renal phenotype

    42. 42 Genetic counseling Goal: Cause of deafness Other medical implication Chance of recurrence in future children Implications for other family members Assist family in making choices that are appropriate for them Team approach including clinical/medical geneticist, genetic counselor, social worker, psychologists Consent need to be obtained for genetic testing

    43. 43 Cochlear gene therapy Adenoid associated virus as vector Routes of delivery Safety concern Hearing loss Regional and distal dissemination

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